Abstract
A large number of colorectal cancers have a genetic background in China. However, due to insufficient awareness, the diagnostic rate remains low and merely 5-6% of colorectal cancer patients are diagnosed with hereditary colorectal cancer. Familial adenomatous polyposis (FAP) is an autosomal dominant genetic disease caused by mutations in the adenomatous polyposis coli (APC) gene. Different mutation sites in APC are associated with the severity of FAP, risks of carcinogenesis, and extraintestinal manifestations. We used next-generation sequencing (NGS) and capture techniques to screen suspected mutation points in the proband in this pedigree. Using modified Sanger sequencing, we identified members of the family who were carriers of this variant and whether this segregated well with disease occurrence. FAP family members had multiple adenomatous polyps in their gastrointestinal tracts, some of which developed into cancer with age. Two subjects presented a rare common bile duct polyp phenotype. No extraintestinal manifestations were observed. A heterozygous frameshift mutation in APC exon 16 (NM_000038.6) was observed in the proband and in other patients: c.3260_3261del (p.Leu1087GlnQfs∗31) (rs587782305); the variant call format was CCT/C. Due to the deletion of two bases, a stop codon appeared after 31 amino acids, and the protein was truncated prematurely, which affected the conformation of the protein. Pedigree genetic linkage analysis showed that the clinical phenotype cosegregated with the APC mutation p.L1087fs. This mutation may be the pathogenic in this FAP family and responsible for this rare common bile duct polyp.
Highlights
In China, the morbidity and mortality rates of colorectal cancer have been on a rise; many of these cases have a genetic background
Hereditary colorectal cancer characterized by polyposis includes familial adenomatous polyposis (FAP), Peutz– Jeghers syndrome (PJS), juvenile polyposis syndrome (JPS), and serrated polyposis syndrome (SPS); it can be further divided into classical FAP (CFAP), attenuated FAP (AFAP), MUTYH-associated polyposis (MAP), Gardner syndrome, and Turcot syndrome subtypes
Pathology investigations after total colon + partial rectal resection revealed stage II tubular adenocarcinoma of the large intestine, with perineural invasion, vascular cancer thrombi, and invasion of the subserosal layer accompanied by extensive adenoma polyps in the large intestine. ree out of 28 lymph nodes from the large intestine exhibited cancer metastasis
Summary
In China, the morbidity and mortality rates of colorectal cancer have been on a rise; many of these cases have a genetic background. Only 5-6% of patients are diagnosed with hereditary colorectal cancer in China [1]. Due to the inadequate awareness regarding this disease in China, the actual rate of hereditary colorectal cancer remains low. Hereditary colorectal cancer characterized by polyposis includes familial adenomatous polyposis (FAP), Peutz– Jeghers syndrome (PJS), juvenile polyposis syndrome (JPS), and serrated polyposis syndrome (SPS); it can be further divided into classical FAP (CFAP), attenuated FAP (AFAP), MUTYH-associated polyposis (MAP), Gardner syndrome, and Turcot syndrome subtypes. FAP was first reported in 1925 [3] It is a special type of hereditary colorectal cancer characterized by a highly explicit autosomal dominant inheritance. FAP manifests as a diffuse growth of hundreds or thousands of adenomatous polyps in the colorectal mucosa, without observable early symptoms
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
